Prion protein NMR structures of elk and of mouse/elk hybrids

Gossert, Alvar D.; Bonjour, Sophie; Lysek, D.A.; Fiorito, Francesco; Wüthrich, Kurt

doi:10.1073/pnas.0409008102

Cited by 250 publications

(303 citation statements)

References 44 publications

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“…For PrP, the first [8] and most abundant structural information has been obtained by nuclear magnetic resonance techniques (NMR), which has resulted in experimentally derived models of PrP of a wide variety of species [64][65][66][67][68][69][70]. For human and sheep PrP, structures determined by X-ray crystallography have also been reported, both with and without antibodies bound [71][72][73][74][75].…”

Section: The Starting Point: Prp Structures From Experimentsmentioning

confidence: 99%

Molecular Dynamics as an Approach to Study Prion Protein Misfolding and the Effect of Pathogenic Mutations

Kamp

Daggett

2011

Topics in Current Chemistry

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Section: The Starting Point: Prp Structures From Experimentsmentioning

confidence: 99%

Molecular Dynamics as an Approach to Study Prion Protein Misfolding and the Effect of Pathogenic Mutations

Kamp

Daggett

2011

Topics in Current Chemistry

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“…The PrP C structure has been solved by nuclear magnetic resonance (NMR) analysis from recombinant prion protein from a library of vertebrate species [13,21,31,[45][46][47]63]. The global architecture of the various mammalian PrP structures are nearly identical.…”

Section: Prp C Structurementioning

confidence: 99%

“…The global architecture of the various mammalian PrP structures are nearly identical. Intriguingly, elk PrP possesses an extremely well-defined loop connecting the second alpha helix and beta sheet (amino acids 166-175), whereas the homologous region is flexibly disordered in human and bovine PrP C [21]. In the laboratory of Kurt Wüthrich, this loop region has been studied in detail, and the loop is thought to provide structural insights into species barriers for prion disease [12].…”

Section: Prp C Structurementioning

confidence: 99%

“…In the laboratory of Kurt Wüthrich, this loop region has been studied in detail, and the loop is thought to provide structural insights into species barriers for prion disease [12]. Further structural studies in two mutant mouse PrP variants derived from the elk PrP primary structure, mPrP[N174T] and mPrP[S170N, N174T], have confirmed that the defined loop in the elk is due to two amino acid exchanges, as the mPrP[S170N, N174T] has the conformationally identical rigid loop of the elk [21]. It is of great interest to determine whether the loop region of the elk influences TSE susceptibility and CWD transmission to other species.…”

Section: Prp C Structurementioning

confidence: 99%

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A prion disease of cervids: Chronic wasting disease

2008

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-Chronic wasting disease (CWD) is a prion disease of deer, elk, and moose, initially recognized in Colorado mule deer. The discovery of CWD beyond the borders of Colorado and Wyoming, in Canada and as far east as New York, has led to its emergence as a prion disease of international importance. Epidemiological studies indicate that CWD is horizontally transmitted among free-ranging animals, potentially indirectly by prion-containing secreta or excreta contaminating the environment. Experimental CWD transmission attempts to other wild and domestic mammals and to transgenic mice expressing the prion protein of cattle, sheep, and humans have shed light on CWD species barriers. Transgenic mice expressing the cervid prion protein have proven useful for assessing the genetic influences of Prnp polymorphisms on CWD susceptibility. Accumulating evidence of CWD pathogenesis indicates that the misfolded prion protein or prion infectivity seems to be widely disseminated in many nonneural organs and in blood. This review highlights contemporary research findings in this prion disease of free-ranging wildlife.

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“…The conformation of the S2-H2 loop seems to play an important role in PrP C /PrP Sc conversion. (i) Protein X was putatively proposed to target the S2-H2 loop and to promote the opening of the molecule like a lever [54]; (ii) in sheep, mutation Q171R located in the S2-H2 loop confers a resistance phenotype to sheep scrapie [49]; (iii) the conformation of this loop was proposed as the basis of TSE susceptibility differences in domestic animals [41]. Since the separation of H1-S2 from the rest of the protein is a prerequisite unfolding event for oligomerization, all mutations affecting the H1-S2 expansion from the H2-H3 bundle may be involved in the PrP C /PrP Sc conversion as for the human Q217R mutation.…”

Section: Structural Dynamics Of Prp Conversionmentioning

confidence: 99%

Misfolding of the prion protein: linking biophysical and biological approaches

2008

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-Prion diseases are a group of neurodegenerative diseases that can arise spontaneously, be inherited, or acquired by infection in mammals. The propensity of the prion protein to adopt different structures is a clue to its pathological and perhaps biological role too. While the normal monomeric PrP is well characterized, the misfolded conformations responsible for neurodegeneration remain elusive despite progress in this field. Both structural dynamics and physico-chemical approaches are thus fundamental for a better knowledge of the molecular basis of this pathology. Indeed, multiple misfolding pathways combined with extensive posttranslational modifications of PrP and probable interaction(s) with cofactors call for a combination of approaches. In this review, we outline the current physico-chemical knowledge explaining the conformational diversities of PrP in relation with postulated or putative cellular partners such as proteic or non-proteic ligands.

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Prion protein NMR structures of elk and of mouse/elk hybrids

Cited by 250 publications

References 44 publications

Molecular Dynamics as an Approach to Study Prion Protein Misfolding and the Effect of Pathogenic Mutations

Molecular Dynamics as an Approach to Study Prion Protein Misfolding and the Effect of Pathogenic Mutations

A prion disease of cervids: Chronic wasting disease

Misfolding of the prion protein: linking biophysical and biological approaches

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